Use the labels in the right column to find what you want. Or you can go thru them one by one, there are only 15849 posts. Searching is done in the search box in upper left corner. I blog on anything to do with stroke.DO NOT DO ANYTHING SUGGESTED HERE AS I AM NOT MEDICALLY TRAINED, YOUR DOCTOR IS, LISTEN TO THEM. BUT I BET THEY DON'T KNOW HOW TO GET YOU 100% RECOVERED. I DON'T EITHER, BUT HAVE PLENTY OF QUESTIONS FOR YOUR DOCTOR TO ANSWER.

Deans' stroke musings

Changing stroke rehab and research worldwide now.Time is Brain!Just think of all thetrillions and trillions of neuronsthatDIEeach daybecause there areNOeffective hyperacute therapies besides tPA(only 12% effective). I have 493 posts on hyperacute therapy, enough for researchers to spend decades proving them out. These are my personal ideas and blog on stroke rehabilitation and stroke research. Do not attempt any of these without checking with your medical provider. Unless you join me in agitating, when you need these therapies they won't be there.

What this blog is for:

Shortly after getting out of the hospital and getting NO information on the process or protocols of stroke rehabilitation and recovery I started searching on the internet and found that no other survivor received useful information. This is an attempt to cover all stroke rehabilitation information that should be readily available to survivors so they can talk with informed knowledge to their medical staff. It's quite disgusting that this information is not available from every stroke association and doctors group.My back ground story is here:http://oc1dean.blogspot.com/2010/11/my-background-story_8.html

Friday, January 12, 2018

This year will bring a Canada Day for the history books. Only July 1, 2018, recreational marijuana (also called cannabis) will be legalized and regulated in Canada.

This means I can get supplies in 100 miles instead of having to drive 17 hours 29 minutes to Denver. I'm not medically trained so I obviously don't know anything. But I will do marijuana after my next stroke.

https://sciencebasedmedicine.org/medical-marijuana-where-is-the-evidence/
This year will bring a Canada Day for the history books. Only July 1, 2018, recreational marijuana (also called cannabis) will be legalized and regulated in Canada. The federal Cannabis Act
creates a legal framework for producing, possessing and selling
marijuana across Canada, meaning that each Canadian province will set
its own rules to oversee its distribution, subject to federal government
conditions. Provincial and federal governments will share in the
responsibility for the oversight of this new system, and will also share
in the tax revenue. Different provinces are taking different
approaches, similar to how alcohol purchases vary between jurisdictions.
This trend follows what we’re seeing at the state level in the United
States, with different states moving to decriminalize recreational use.

Marijuana has been legal to some extent in Canada (and in many US
states) for some time, in the form of “medical” marijuana. The Canadian
government authorized the sale of marijuana for that purpose, while it
simultaneously emphasizes that cannabis is not an approved therapeutic
product. The medical market, for many, appears to simply be a means to access products for recreational, or non-medical use, and has generated wildly unsubstantiated claims about the medical merits of marijuana for conditions like autism and the treatment of cancer.
Dispensaries have appeared across Canada and the US, usually with very
easy referrals for prescriptions. Some dispensaries ignore any
prescription requirement entirely and will sell marijuana directly to
the public without any medical assessment or advice. With the
introduction of government-overseen (and in some Canadian provinces,
government-delivered) retail sales in Canada later this year, it’s
reasonable to assume that unregulated dispensaries will eventually
disappear.

With recreational sales imminent in Canada (and already here, in states like California),
there are questions about the future market for “medical” marijuana.
Should use for medical purposes be treated like recreational use, where
consumers make their own selections, and purchases are taxed like other
consumer products? Or should some forms or uses of marijuana be treated
like prescription drugs, where a health professional remains involved,
and products may be even be covered by insurance plans? Given the major
changes we are seeing in how we can access marijuana, it’s worth
summarizing the current state of evidence for marijuana when used for
specific medical purposes. With marijuana becoming much more accessible,
physicians, other health professionals, and their patients need
high-quality information about its value for different medical
conditions. David Gorski reviewed much of the evidence
in a series of posts over the past three years. Now, three new
documents prepared for Canadian physicians and health professionals
concisely summarize the current evidence base for medical marijuana.

The pharmacy profession seemingly sees a bright future in medical marijuana, with big chains striking deals with producers and even hiring “brand managers”
in anticipation of the shuttering of unregulated dispensaries and a
continued demand for “medical” uses. The argument being made by the
pharmacy profession seems to be that (1) marijuana is a legitimate drug
for medical purposes, and should be treated as such, which includes (2) a
pharmacy and pharmacist being involved in the provision. The latter we
can set aside for now, and focus first on whether or not marijuana is
indeed a drug that should be treated like other prescription drugs.

Before I continue, I should state my personal position on marijuana. I
am fully supportive of the legalization of marijuana for recreational
use and support regulation and taxation, treating it along the lines of
alcohol or tobacco. I should also state that I have no “skin in the
game” when it comes to marijuana in pharmacies, or medical marijuana
more generally – I don’t work in retail pharmacy, and while pharmacy
professional associations seem enamored with the idea of medical
marijuana in pharmacies, I have no personal opinion on it, other that
wanting pharmacies to be places that offer and promote science-based and
medically useful products, not pseudoscience or harmful/ineffective
products (see my post on the commercial and professional ethical obligations of pharmacists for more).

It’s worth mentioning as an aside that there’s a somewhat similar set
of circumstances in US history, when alcohol was available only by
prescription during Prohibition. This prescription (via the Smithsonian Institute) could be used by physicians to prescribe alcohol for an array of ailments:

Naturally, the prescription market for alcohol disappeared once
Prohibition ended. But marijuana is not alcohol. It contains an array of
potentially medically useful chemical substances, several of which have
been clinically investigated for the treatment of different medical
conditions.

The pharmacology of marijuana

As David Gorski has pointed out in previous posts,
there are a number of biologically active chemicals in marijuana. The
main psychoactive ingredients are called cannabinoids, and the primary
cannabinoid produced is delta-9-tetrahydrocannabinol (Δ9-THC,
or simply THC.). Cannabinoids are produced in the stalk, leaves,
flowers, seeds and resin of marijuana plants. Marijuana can be smoked,
vaporized, and eaten, among other forms of ingestion. THC is rapidly
absorbed, and when inhaled, reaches the brain within minutes. (Oral
absorption is lower owing to a significant reduction in available drug
after passing though the liver.) These chemicals bond to cannabinoid
receptors on cells throughout the body, triggering or modulating
different effects. Marijuana immediately affects and impairs attention,
concentration, memory, learning and motor coordination, proportional to
the dose. You might wonder why our cells have receptors for THC and
other cannabinoids. That’s because we (and other mammals) have an endocannabinoid system,
and we naturally produce enocannabinoids. It is absolutely plausible
that drugs that target endocannbinoid receptors, like THC (or
derivatives), have the potential to produce beneficial medicinal
effects, given the presence of receptors on nearly every organ system.
With the growing understanding of the endocannabinoid system, and the
identification of different types of receptors, there’s the potential
for targeting specific effects on specific organs. That could mean
products that produce beneficial effects and minimize any adverse
effects (e.g., fewer psychoactive effects).

Cannabinoids are highly fat soluble and so are difficult for the body
to eliminate – the complete elimination of a single dose may take up to one month.
With repeated doses, levels can rapidly accumulate. While the liver
eliminated cannabinoids, even the metabolites of THC can persist in the
body, and there is little relationship between the levels of THC found
in the blood and the degree of THC-induced effects. Owing to metabolism
in the liver, THC has the potential to interact with other drugs. The
overall impact has not been well studied. As a drug, there is lot we do
not know about marijuana. However, we can be confident in observing that
there is little acute toxicity of marijuana, unlike many other drugs
and substances. While not addictive, there are also cases of cannabis
use disorder, which while infrequent, can occur. It should be
acknowledged that cannabis use disorder is a minor public health issue
compared to the widespread harms and mortality caused by substances like
alcohol and opioids.

Are medical cannabinoids (MC) effective for the treatment of pain?

Bottom Line: Evidence for inhaled marijuana for pain is
too sparse and poor to provide good evidence-based guidance. Synthetic
MC-derived products may modestly improve neuropathic pain for one in
11-14 users but perhaps not for other pain types. Additionally, longer
and larger studies (better evidence) show no effect. Adverse events are
plentiful.

Chronic pain: 39% experience pain reduction of
>30% versus 30% with placebo, resulting in a number needed to treat
(NNT)=11. Larger and longer RCT show no effects. The mean pain
improvement is 0.5 on a 0-10 scale, which isn’t clinically meaningful.

Neuropathic pain: With inhaled MC, the NNT=6. With any MC, the NNT=14.

Pain from multiple sclerosis: Mean pain improvement over placebo was 0.8 on a 1-10 scale which was borderline insignificant.

Acute pain: One positive trial, one negative trial, and five trials showing MC is equivalent to placebo.

When compared to medication, MC was no better than amitriptyline
(with more adverse events), or worse than dihydrocodeine with similar
adverse events.

No overall differences shown in quality of life.

Little evidence for back pain, fibromyalgia, or osteoarthritis.

What are the harms associated with medical cannabinoid therapy?

Bottom Line: Compared to placebo, medical cannabinoids
cause multiple different adverse events in patients, from visual
disturbance or hypotension (1 in 3-10) to hallucination or paranoia (1
in 20). Stopping due to adverse effects occurs in 1 in every 8-20
patients. Regardless of the type of medical cannabinoid used, adverse
events are common and likely underestimated. Given the extensive harms,
potential benefits must be impressive to warrant a trial of therapy.

79-92% of patients using MC experienced any adverse event versus 56-78% with placebo, giving a number needed to harm (NNH)=5-8.

Serious adverse events measured in 3 meta-analyses, with two studies
reporting no significant differences versus placebo. The third reported
an odds ratio of 1.41.

Seven meta-analyses reporting stopping MC due to adverse events,
with a range of 7-14% for MC versus 1-5% for placebo, giving an
estimated NNH of 8-22. One of the seven analyses showed no significant
difference versus placebo.

In other conditions, high level evidence is sparse, low quality, or
negative, for conditions such as glaucoma, anxiety, or other causes of
nausea and vomiting.

Bliniding in trials was noted to be difficult, with 85-95% of patients and clinicians identifying who receiving MC.

Developing an evidence base for marijuana

Studying marijuana under rigorous circumstances has been difficult
until fairly recently. The plant itself isn’t patented, so even ignoring
the legal access issues, there may be a lack of industry enthusiasm in
conducting clinical trials. The other issue is the challenge of a proper
placebo control, particularly for non-oral forms of use. Given the
psychoactive effects and the widely heralded effects on conditions that
can only be assessed subjectively, like nausea, fatigue or appetite, a
proper placebo is essential to separate out actual from placebo effects.
While some commercial products have been developed and marketed with
standardized ingredients and quality control (e.g., nabilone),
these products are exceptions. However, these purified and standardized
products have allowed for proper placebo controls and more rigorous
assessments of effectiveness. Regrettably, these products haven’t been
shown to be that effective which may suggest that the perceived
beneficial effects may be largely placebo effects. Hopefully, clinical
trials will become more common and more marijuana-based drugs can be
more rigorously evaluated.

Conclusion: Evidence is lacking

The use of psychoactive drugs like marijuana is a health issue,
particularly when used for medical purposes. Regrettably, there is a
lack of high-quality data that shows marijuana for most medical purposes
is both safe and effective. What little evidence exists is of poor
quality and may not even be representative of the purposes for which
medical marijuana is sought. There are significant gaps in information
necessary to treat marijuana like other forms of medicine: Dosage
standardization and overall quality control may not be in place. Overall
effectiveness, contraindications, drug interactions, adverse events and
long-terms risks when marijuana is used as medicine are not well
understood. The best evidence suggests that marijuana may be a
reasonable treatment option only when safer, more effective, and better
tolerated treatment options have been tried first. If marijuana is to be
treated as medicine, then it needs to meet the same standards of
quality, effectiveness, and safety we would expect of any other
prescription drug. That standard has not yet been met.

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Canoeing Moose

Just because my goal is to get back to canoeing and this moose is so ripped and cool looking. And he's even a solo paddler. But his right hand on the T-grip is wrong and the right arm should be extended.